HPV Vaccine Debate in South Africa#android#iPad#retweet

By Norma Erickson

9 August 2015, a citizen of South Africa (we’ll call her Sarah) sent the following questions about HPV vaccines to CANSA, the Cancer Association of South Africa. Sarah had no idea her questions would lead to a full-blown scientific debate.

Could you please let me know why CANSA is supporting the use of the hpv vaccines when these are now proven to be deadly? Several hundred young women have died because of this vaccine and thousands more are permanently disabled or battling with chronic health-problems. This vaccine has NEVER been proven to prevent cervical cancer. Many countries have banned these vaccines because they are not just useless, they are dangerous – why is South Africa using them? And why does your web page not list the potential side effects?

Sarah received a reply on August 13th referring her to Professor Michael Herbst, a clinical expert who would answer her questions. Professor Herbst sent Sarah copies of 5 abstracts from peer-reviewed scientific journal articles which stated the following. (CANSA Correspondence: Complete copy here, begins on page 3)

  • …trials have proven its (HPV vaccine) efficacy in preventing cervical intraepithelial neoplasia (CIN) beyond doubt and its effectiveness in preventing cervical cancer though presumptive is reasonably certain as per mathematical modelling. It also prevents other HPV related anogenital and oropharyngeal malignancies in both sexes.
  • The HPVs vaccine prevents infection with certain species of HPVs associated with the development of cervical cancer, genital warts, and some less common cancers.
  • The cost-effectiveness of human papillomavirus (HPV) 16/18 vaccination of 12 year-old girls was calculated for 28 countries, under the assumption that vaccination prevents 70% of all cervical cancer cases and that cervical cancer and all-cause mortality rates are stable without vaccination. At three-dose vaccination costs of I$ 100 per vaccinated girl (currency 2005 international dollars), HPV16/18 vaccination was very cost-effective in 25 out of 28 countries…
  • Human papillomavirus (HPV) infection is a central and necessary, although not sufficient, cause of cervical cancer. Besides HPV, the additional multiple risk factors related with the onset of cervical cancer are early-age sexual activities; high number of sexual partners, which is the most salient risk factor; suppression and alteration of the immune status; long-term use of oral contraceptives; and other hormonal influences.
  • Our analysis (of 24 Hispanic mothers/28 daughters) found several themes that affect whether Hispanic girls get the HPV vaccine: gaps in knowledge; fears and concerns about the vaccine; sociocultural communication practices; and decision-making about HPV vaccination. Both mothers and girls had limited knowledge about cervical cancer, HPV, and the vaccine.

As you can clearly see, Professor Herbst’s reply did not address any of the questions Sarah had asked. Undaunted, she replied to him on August 16th as follows (excerpts):

Dear Prof Herbst

Thank you for the document containing various abstracts to papers on the subject of HPV. With all due respect, these are obviously of zero value in terms of answering the questions that I put to CANSA.

My specific questions are:-

Why is CANSA supporting the use of the HPV vaccines when these are now proven to be deadly and when they have NEVER been proven to prevent cervical cancer? Both India and Japan have stopped giving this vaccine because of the severe side effects – why is South Africa ignoring the glut of data that shows this vaccine is dangerous? (Followed by multiple reference documents)

What we do need to do is look at the reported adverse events and to ask the pertinent questions regarding the safety of this vaccine. No manufacturer is going to admit (unless forced to by a court of law) that their product is either defective or deadly.

If anyone purports to be a caring physician and who wishes to help the community defend itself against deadly diseases, then surely that person needs to look at both sides of the argument? It is completely unacceptable simply to point towards the manufacturer and trust that their data is 100% accurate. Attached is a document that lists many of the criminal activities of (and fines handed down to) various pharmaceutical companies. These are the reasons why a good proportion of the general public does not trust the pharmaceutical industry.

Patients have a right to know the risks and benefits of any medical treatment offered to them. Attached is a document that gives pertinent information for South Africans, including the issue of informed consent. This information should be made known to the patient BEFORE the administration of this vaccine.

I therefore respectfully ask that you go through the above information and then kindly answer my questions.

Several emails were exchanged over the next few days, culminating with this request to Sarah from Professor Herbst on August 20th:

Please forward to CANSA any scientific evidence (unbiased peer-reviewed research) / scientific reference that supports and proves that:

  • HPV vaccines are deadly
  • That several hundred women have died as a direct result of the vaccine (please reference country / countries where women have died & number of women who have died)
  • That the HPV vaccine was directly responsible for the disability / disabilities that are claimed to result from HPV vaccine (include disability type, numbers affected and country)
  • That there is a direct link between HPV vaccine and the chronic health problems you refer to (specific chronic conditions, numbers affected and country) Please forward scientific information regarding the banning of HPV vaccine by different countries together with the scientific grounds on which the vaccine was banned – please also identify the countries by name.

Find attached a few abstracts of peer-reviewed scientific research which categorically state that HPV vaccine prevents cervical cancer and Google ‘PubMed’ and then the key words “HPV vaccine Cervical Cancer Prevention” and read further scientific evidence supporting this.

Professor Herbst had been very careful in the wording of his request to Sarah. He knew, or should have known, exactly how difficult it would be to prove HPV vaccines have been the direct cause of any permanent disability or death. Sarah was not intimidated. She took on the challenge.

By 13 September 2015, she sent Professor Herbst an email with a 105-page document, complete with references from around the world to back up her personal concerns regarding HPV vaccines and vaccination programs. (Read Sarah’s CANSA Reply September 2015 here.)

As of November 15th Sarah had not received a reply from anyone at CANSA, so she sent a short email reminding them she was not going away. She stated she intended to pursue the matter and go public with the truth about how she had been treated with regard to the HPV vaccine matter.

17th November, Professor Herbst had CANSA’s Information Coordinator send Sarah a copy of the CANSA’s Fact Sheet on Human Papillomavirus Infection and Cancer. (Pages 19-32 of this document)

6th December, Sarah responded to the latest email stating:

Thank you for the email from Radiah but there was no response from you to my questions. Attached was a document that is merely standard information and which contains gross inaccuracies such as:-

“Are the HPV vaccines safe and effective? Both the vaccines as said to be safe and effective. Both vaccines were tested in thousands of people around the world. These studies showed no serious side effects. Common, mild side effects included pain where the shot was given, fever, headache, and nausea. As with all vaccines, CDC and FDA continue to monitor the safety of these vaccines very carefully.”

Clearly the above is not a response from you but is just a regurgitation from the manufacturer.

Where is the scientific evidence behind “both the vaccines are said to be safe and effective”? Who said they are “safe and effective”? Where is the evidence to back up this claim?

Approximately two and a half hours later, Professor Herbst responds with the following message:

Dear Ms XXX

March 12, 2014 Global Advisory Committee on Vaccine Safety Statement on the continued safety of HPV vaccination as with all new vaccines, the Global Advisory Committee on Vaccine Safety has been reviewing the safety of HPV vaccines since they were first licensed in 2006. The World Health Organization (WHO) recommends the introduction of HPV vaccination into national immunization programmes where prevention of cervical cancer is a public health priority and the introduction is programmatically feasible [1]. While early detection of pre- and cancerous cells through screening programs has helped decrease incidence rates of cervical cancer in women aged 25-45 in the UK, for example [2], that decrease has plateaued in the past decade. While safety concerns about HPV vaccines have been raised, these have systematically been investigated: to date, the GACVS has not found any safety issue that would alter any of the current recommendations for the use of the vaccine.

The purpose of this update is to summarize the work of GACVS over the past six years in reviewing the safety of HPV vaccines. It is important to highlight and reiterate this work because a number of national immunization programs have been facing real and potential public losses of confidence in their programs as a result of increased negative publicity, even from safety issues that have been addressed.

To date, the GAVCS has reviewed evidence related to syncope, anaphylaxis, venous thromboembolism, adverse pregnancy outcomes, Guillain Barre Syndrome, and stroke [3]. It also examined concerns around the aluminium adjuvant used in HPV vaccines, with considerations around the toxicology of aluminium adjuvants and studies by investigators claiming that aluminium in the quantities used in vaccines are associated with adverse health outcomes [4]. Finally the Committee also reviewed the question of autoimmune disease, specifically around multiple sclerosis (MS), cerebral vasculitis, and an evolving concern over cases of complex regional pain syndrome (CRPS) and/or other chronic pain conditions following vaccination that have surfaced.

With respect to aluminium, the GACVS has had occasion to review the safety of the adjuvant on several occasions, beginning in 1999. At that time, deltoid muscle biopsies performed in France on a number of patients with a variety of complaints revealed in a small number the presence of a minute inflammatory focus of macrophages with associated necrosis. These localized lesions, called macrophagic myofasciitis (MMF), have been shown to contain aluminium salts [5, 6]. Since the location of the lesions in the deltoid muscle coincides with the usual site of injection for vaccines, these microscopic lesions may appear to be related to immunization. The investigators from the “Groupe d’études et de recherche sur les maladies musculaires acquises et dysimmunitaires” (GERMAAD) have suggested that vaccination and localized MMF lesions might be associated with a multi-system disorder. The GACVS has reviewed evidence regarding MMF on several occasions since that time and continues to reaffirm that, while MMF is clearly linked to a vaccination “tattoo” among some patients who have received an aluminium containing vaccine, the associated systemic symptoms related to that finding have never been scientifically proven. Statements about MMF were published in 1999, 2002 and 2004 [4]. While there have never been any published reports of MMF in recipients of HPV vaccines, there is no plausible reason to suspect that any reports of MMF would be associated with systemic symptoms following aluminium containing HPV vaccines any more than the finding of the histological lesion of MMF following hepatitis B vaccine and clinical symptoms.

In 2012, the GACVS reviewed two studies claiming an association between aluminium in vaccines and autism spectrum disorder [7, 8]. It found serious flaws in the two studies that limited their value even for hypothesis generation. In December 2013, the GACVS reviewed evidence related to HPV vaccine and autoimmune disease, specifically multiple sclerosis [3]. While there remain case reports in the literature, multiple epidemiologic studies have not demonstrated any increased risk of autoimmune diseases, including MS, in studies, some of which have included girls who have received HPV vaccine compared to those who had not [9, 10, 11, 12].

Several papers have also been published pertaining to the finding of HPV L1 gene DNA fragments in clinical specimens following HPV vaccination [13, 14]. These papers claimed an association with clinical events of an inflammatory nature, including cerebral vasculitis. While the GACVS has not formally reviewed this work, both the finding of DNA fragments in the HPV vaccine and their postulated relationship to clinical symptoms, have been reviewed by panels of experts. First, the presence of HPV DNA fragments has been addressed by vaccine regulatory authorities who have clearly outlined it as an expected finding given the manufacturing process, and not a safety concern [15]. Second, the case reports [13] of adverse events hypothesized to represent a causal association between the HPV L1 gene DNA fragments and death were flawed in both clinical and laboratory methodology [16]. The paper described 2 fatal cases of sudden death in young women following HPV vaccine, one after 10 days and one after 6 months, with no autopsy findings to support death as result of cerebral vasculitis or an inflammatory syndrome. Thus the hypotheses raised in these papers are not supported by what is understood about the residual DNA fragments left over following vaccine production [17]: given the extremely small quantities of residual HPV DNA in the vaccine, and no evidence of inflammation on autopsy, ascribing a diagnosis of cerebral vasculitis and suggesting it may have caused death is unfounded.

In June 2013, the GACVS reviewed the concerns arising in Japan in regard to reports described as CRPS in a few cases, and other chronic pain conditions following HPV vaccine. At the time, GACVS found no evidence to suggest a causal link with the HPV vaccine, and recommended careful documentation of each case and definition of diagnostic criteria to guide management and causality assessment. The Committee has meanwhile continued to monitor the HPV vaccine and considered further issues during their meeting in December 2013 [3]. In Japan, an expert advisory committee has continued to meet and review the situation but has not yet reached a conclusion. It is acknowledged that the HPV vaccine may be a more painful injection, leading to frequent complaints of pain, which, in some settings, may trigger additional non-specific complaints [18, 19]. As to Complex Regional Pain Syndrome, this entity has been described following various forms of trauma, including injury, surgical procedures and injections. It is therefore plausible that CRPS could develop following the injection of any vaccine (however, such cases have been very rarely described in the literature [20]).In summary, the GACVS continues to closely monitor the safety of HPV vaccines and, based on a careful examination of the available evidence, continues to affirm that its benefit-risk profile remains favorable. The Committee is concerned, however, by the claims of harm that are being raised on the basis of anecdotal observations and reports in the absence of biological or epidemiological substantiation. While the reporting of adverse events following immunization by the public and health care providers should be encouraged and remains the cornerstone of safety surveillance, their interpretation requires due diligence and great care. As stated before, allegations of harm from vaccination based on weak evidence can lead to real harm when, as a result, safe and effective vaccines cease to be used. To date, there is no scientific evidence that aluminium-containing vaccines cause harm, that the presence of aluminium at the injection site (the MMF “tattoo”) is related to any autoimmune syndrome, and that HPV DNA fragments are responsible for inflammation, cerebral vasculitis or other immune-mediated phenomena.

Prof Michael C Herbst

Health Specialist

[D Litt et Phil (Health Studies); D N Ed; M Art et Scien; B A Cur; Dip Occupational Health]

Cancer Association of South Africa – Head Office
Address: 26 Concorde Road West, Bedfordview, 2008
Postal: PO Box 2121, Bedfordview, 2008

December 7th, excerpts from Sarah’s response:

It greatly concerns me that CANSA appears to have no thoughts of its own and instead relies on statements from organisations who have a vested interest in pursuing vaccination programs and maintaining “public confidence”.

Upon reading the GACVS statement, anyone who had not investigated this matter would think that this vaccine is perfectly safe, yet the truth is far from that as can be seen by the various protest groups, lawsuits, representations to governments and other actions being taken by victims of the HPV vaccines. If the vaccine was perfectly safe, why are SO many victims stepping forward and why are many, many doctors, scientists and health professionals trying to get their message heard about the dangers of these vaccines? So in other words, the manufacturers are relying on voluntary reports to reveal adverse reactions ‘post marketing’.

To which Professor Herbst responds on December 8th with:

Dear Ms XXXXX Thank you for your response. I wish to inform you that I am ending our discussion on HPV vaccination. If you have issues around HPV vaccination, I would like to suggest that you take it up with the National Department of Health, and not with the Cancer Association of South Africa.

Kind Regards, Prof Michael C Herbst Health Specialist

Sarah responds almost immediately with (page 39):

I am saddened and appalled at your response. I am a cancer survivor myself (malignant melanoma) and I am shocked that CANSA refuses to answer genuine concerns about a pharmaceutical product that is supposed to protect against cancer. The general public is led to believe that organisations like CANSA have the best interests of the public at heart but clearly this is not the case.

I therefore wish to place on record the following conclusions that I have drawn from the lack of response by CANSA:

  1. CANSA has no interest in protecting the lives of females (or males, as young males are now also being drawn into the HPV vaccination program) in South Africa
  2. CANSA is unwilling to properly investigate the flood of reports, scientific studies and documented evidence of the dangers of HPV vaccines
  3. CANSA is not providing balanced information to the general public of the dangers of HPV vaccines and therefore has no interest in ensuring full informed consent
  4. CANSA refuses to answer my concerns and questions
  5. CANSA is putting the lives of all young South Africans at risk by failing to properly investigate the devastating serious adverse effects that are being reported all over the world

As much as Professor Herbst would have liked this to be the end of his conversation about HPV vaccines, it was not meant to be. During the course of Sarah’s communications with the director of CANSA, one of the scientists whose work was criticized in Professor Herbst’s Dec 6th email had an opportunity to read what the professor had stated. Consequently, Dr. Sin Hang Lee responded directly to Professor Herbst via email (complete email with references here.) on December 11th as follows:

Dear Professor Herbst:

Based on your 06 December 2015 letter addressed to Ms XXXX on behalf of the Cancer Association of South Africa, you are obviously not a scientist, but are trying to dismiss a very important scientific issue which has affected the health of many teenagers worldwide. Since you are masquerading as a health specialist, acting as a spokesman in a cancer association and trying to discredit my scientific work on the finding of HPV L1 gene DNA in the vaccine Gardasil® while using your position to influence health policy decision making according to your agenda, your letter must not be allowed to pass without challenge.

The first exposure of your lack of understanding of the science involved in this matter is contained in your statement “Several papers have also been published pertaining to the finding of HPV L1 gene DNA fragments in clinical specimens following HPV vaccination [13, 14]. These papers claimed an association with clinical events of an inflammatory nature, including cerebral vasculitis.”

You quoted as reference #13 a paper published by “Tomljenovic L, Shaw CA. Death after Quadrivalent Human Papillomavirus (HPV) Vaccination: Causal or Coincidental? Pharmaceut Reg Affairs 2012, S12:001”. If you had understood what HPV L1 gene DNA fragments mean, you would not have made such an erroneous statement as you did because in their entire paper, Tomljenovic and Shaw never mentioned “HPV L1 gene DNA fragments” even once. These authors demonstrated HPV-16L1 VLPs, not DNA fragments in the blood vessel walls. You obviously do not understand the difference between HPV L1 VLPs and HPV L1 gene DNA fragments.

You quoted as reference #14 a paper published by “Lee, SH. Detection of human papillomavirus L1 gene DNA fragments in postmortem blood and spleen after Gardasil® vaccination— A case report. Advances in Bioscience and Biotechnology, 2012, 3, 1214-1224”. You are basically putting your words into the author’s mouth because I know the author did not claim cerebral vasculitis in this case report.

In an attempt to boost your credibility, your also wrote “….the case reports [13] of adverse events hypothesized to represent a causal association between the HPV L1 gene DNA fragments and death were flawed in both clinical and laboratory methodology [16].”  For reference 16, you cited a CISA Technical report from a U.S. CDC webpage.

However, in this CDC technical report, the unnamed authors of the document only questioned the HPV-16L1 particles, never HPV L1 gene DNA fragments. Therefore, it further confirms the fact that you really do not understand these two important and distinct chemicals in the HPV vaccine at all. And there is a Disclaimer following this document, stating: The information and conclusions in this report are those of the work group participants addressing this issue and do not necessarily represent the official position of CDC. So you blindly misquoted a technical report written by a team of ghost writers to dismiss a potential causal association between the HPV L1 gene DNA fragments and death.

You were unable to find a scientific publication published in a peer-reviewed journal to challenge the plausible mechanism leading to potential harm induced by residual HPV DNA left in the vaccine Gardasil®. So you had to use a blog written by a Dr Helen Petousis-Harris who knows even less than you do on this subject to support your opinion. In her blog (your reference #17), Dr Helen Petousis-Harris did not even cited a single publication of mine, and used some social media articles published on the Internet to attack me by character assassination. Although she had no personal experience on viral DNA research, she was brave enough to declare that the quantity of residual HPV DNA left in the vaccine Gardasil® has no health impacts on the vaccinees. It is unfortunate for the teenagers of this world to have people like you and Dr Helen Petousis-Harris to rely on selling your biased opinions without any scientific evidence of your own to influence health policy decision making. Neither of you has done any work to support your opinions. Neither of you knows what you are talking about. If you want to prove me wrong, please show me a report of the amount of HPV L1 gene DNA fragments (type 16, 11, 18 and 6) which are bound to the aluminum adjuvant, as found in the vaccine Gardasil® that has been shown to be of no short-term or long-term risk to humans.

Since you have quoted in your reference #12, a paper published by Slade BA, Leidel L, Vellozzi C, Woo EJ, Hua W, et al. Postlicensure safety surveillance for quadrivalent human papillomavirus recombinant vaccine. JAMA. 2009 Aug 19; 302(7):750-7. Let me point out to you that this CDC study shows that among 12,424 reported adverse events following Gardasil® vaccination from June 1, 2006 through December 31, 2008, there were 32 deaths with a mean age of 18 years old, who died 2 to 405 days after the last Gardasil® injection. Medical records and autopsy reports on 20 of the 32 deaths were available for review and confirmed there were 4 unexplained deaths and 6 cardiac-related deaths.

This same report also stated that syncope is the most common adverse reaction after Gardasil® injections and “The reporting rates per100 000 qHPV doses distributed were 8.2 for syncope;”

Syncope is defined as temporary loss of consciousness and posture, described as “fainting” or “passing out.” It’s usually related to temporary insufficient blood flow to the brain. It most often occurs when the blood pressure is too low (hypotension) and the heart doesn’t pump a normal supply of oxygen to the brain.

In view of the high incidence of syncope developed among Gardasil® vaccinees, the FDA Prescribing Information for Gardasil® (qHPV) contains the following Warnings and Precautions:

“Because vaccinees may develop syncope, sometimes resulting in falling with injury, observation for 15 minutes after administration is recommended. Syncope, sometimes associated with tonic-clonic movements and other seizure-like activity, has been reported following vaccination with GARDASIL®. When syncope is associated with tonic-clonic movements, the activity is usually transient and typically responds to restoring cerebral perfusion by maintaining a supine or Trendelenburg position.”

So why do Gardasil® vaccinees have a higher rate of syncope as compared to other vaccinees? The ugly truth that you and those agencies you have quoted to support your biased opinions would not like to face may be in the HPV L1 gene DNA fragments when the viral DNA fragments combine with the aluminum adjuvants in the vaccines. To understand this, you really have to spend time to study the history on the science of aluminum adjuvants in vaccination.

Aluminum salts have been used as adjuvants in vaccination empirically to boost immune responses of the host to the protein antigens for many decades. However, the mechanism of the adjuvant effects of aluminum salts has only been recently investigated at the molecular level.  It is now generally agreed in the scientific community that aluminum salts used as adjuvants are toxic and always damage the cells of the host at the site of injection, causing a localized inflammation at the vaccination site. This initial cell damage by the aluminum salt is an essential and necessary step to initiate its adjuvant effects because the free host DNA molecules released from the aluminum salt-damaged host cells act as mediators to trigger augmented immune responses of the host [1, 2]. The free DNA molecules of the dying host cells, also referred to as damage-associated molecular patterns (DAMPs) [3] bind the aluminum salt adjuvant at the site of injection, and the resulting DNA/aluminum complexes are phagocytized by the antigen-presenting cells (APCs) and macrophages. It was known as early as 2003, that when bound to aluminum salts as nanoparticles, free DNA molecules undergo dramatic conformational changes and can be introduced into mammalian cells as a means of gene transfection [4]. In vaccination with aluminum adjuvants, the transfected host DNA activates the pathways that would increase their ability to interact productively with antigen-specific CD4 T cells to boost host immune responses [1, 2]. In plain language, free DNA derived from the dying host cells is needed to be carried by aluminum adjuvants into the APCs or macrophages to function as mediators for boosting immune responses in vaccination.

However, the presence of recombinant HPV L1-specific DNA fragments in the vaccine Gardasil® has disrupted this expected normal immunity response platform in vaccination. The HPV DNA molecules, being of a viral origin, are “non-self” microbial products, also referred to as pathogen-associated molecular patterns (PAMPs). The human body’s defense system can distinguish the PAMPs from the DAMPs in order to mount an appropriate immune response to either the presence of a pathogen or a tissue damage [3].

The amorphous aluminum hydroxyphosphate sulfate (AAHS) nanoparticles which are expected to bind the free host DNA at the site of vaccine injection can also bind the fragments of HPV L1 gene DNA present in the vaccine Gardasil® [5] through a ligand exchange process between the phosphate groups of the DNA molecule and the hydroxyl groups on the aluminum adjuvant surface, similar to a reaction between phospholipids and AAHS in the recombinant hepatitis B vaccine [6]. In other words, Gardasil® has been furnished with a set of ready-made instant DNA immune “mediators” already in the adjuvant, in the form of a viral DNA/aluminum chemical compound, specifically an HPV L1 gene DNA/AAHS complex. The downstream events after transfection into the human macrophages of these viral DNA fragments which are rarely found in the human genome [7] are quite different from those after the DNA of the dying host cells is introduced into the macrophages. Despite similarities between DNA molecules, mammalian cells have the remarkable ability to distinguish viral DNA from their own DNA. The human macrophages are able to recognize the HPV L1 gene DNA as a ‘stranger’ and a ‘danger’ signal, and in response produce many antiviral immune molecules, collectively referred to as type I interferons and pro-inflammatory cytokines [8-10].

Massive systemic production of these type I interferons and pro-inflammatory cytokines induces an antiviral state and protects the host, but it also can contribute to endotoxin lethality and autoimmune diseases [9]. Many of these cytokines are myocardial depressants. The two cytokines that show the greatest cardiovascular effects in animals and humans are tumor necrosis factor (TNF)-α and IL-1β [11]. Administration of recombinant TNF-α in animal models is known to cause hemodynamic changes and even death [11].

Injection of Gardasil® into animals has been shown to induce unusually early strong innate immune responses with quick releases of a variety of cytokines from the macrophages [12]. Injection of HPV DNA/AAHS complexes into the host is also known to induce a strong immune reaction and a strong CD8 T cell response [13].  Based on experiments with other viral DNA molecules, the recombinant HPV L1 gene DNA fragments transfected into human macrophages would also be recognized as “stranger” and “danger” signal, and invariably activate the macrophages to release numerous antiviral cytokines. Many of these cytokines, including TNF-α and IL-1β, are recognized myocardial depressants [14-18]. Hypotensive shock induced by TNF-α has been well documented among animals [19, 20] and humans [21, 22].

This brief review of literature shows that there is a known molecular mechanism to explain why syncope occurs more often in people injected with Gardasil® than with other vaccines, and why certain predisposed vaccinees may suffer a sudden unexpected death as the result of Gardasil® vaccination. You and those who blindly dismiss the potential toxicity of aluminum adjuvant and in particular the toxicity of the newly created HPV L1 gene DNA/AAHS compound for marketing an HPV vaccine should be held responsible for intentionally ignoring the scientific evidence at the expense of public interest.

It is of interest that you mentioned that in June 2013, the GACVS reviewed the concerns arising in Japan in regard to reports described as CRPS in a few cases, and other chronic pain conditions following HPV vaccine. But you apparently purposely avoided mentioning the facts that the Japanese government has suspended its HPV vaccine recommendation since 2014 and that a December 10, 2014 Symposium held by the Japan Medical Association and the Japanese Association of Medical Sciences concluded that HPV vaccines should be promoted only after issues regarding vaccine safety are settled.

In summary, to protect the health of the young children there is an urgent need for open debate of the risks versus benefits of HPV vaccination being recommended or forced onto the 12-year old school girls and boys. A simple declaration of vaccine safety made by some armchair professor like you does not serve the interest of the public.

Sin Hang Lee, MD, F.R.C.P. (C), FCAP

Director, Milford Molecular Diagnostics Laboratory

2044 Bridgeport Avenue, Milford, CT 06460 USA

The following is an excerpt from Professor Herbst’s email (link to entire email) reply to Dr. Lee which was sent on December 11th:

I wish to thank you for the information provided by you. I undertake to include your counter arguments and other relevant information supplied by you in an updated version of CANSA’s Fact Sheet on Human Papilloma Virus Infection and Cancer when our offices re-open on 4 January 2016 and will forward a copy of the updated document to you. I will also google your other research contributions in this regard.

There you have it – one single individual putting forth honest questions and demanding honest, documented answers can make a difference!

If Professor Michael Herbst lives up to his word and alters the CANSA fact sheet on HPV infection and cancer to reflect Dr. Lee’s concerns, the women of South Africa will be able to understand the potential risks of HPV vaccines as well as the potential benefits prior to making a decision as to whether or not HPV vaccines are a good addition to their cervical cancer prevention program.

The women of South Africa will be able to exercise their right to informed consent, thanks to Sarah.

This article in it’s entirety, is compliments of Sane Vax

Vaccine Injury Compensation Program: Fatality after Gardasil#android#iPad#retweet

By Norma Erickson

SaneVax-FeaturedGardasil®-related fatal myocardial infarction in a teenage boy – case filed in United States Court of Federal Claims Office of Special Masters.

Gomez versus USDOH: Petition No. 15-0160V1 filed by the Roberts Law Firm of Newport Beach, California for petitioners Adan Gomez and Raquel Ayon, on behalf of their deceased son Joel Gomez, states:

Joel Gomez received a Merck Gardasil vaccine on June 19, 2013 and again on August 19, 2013, and died in his sleep the following day on August 20, 2013. The death was caused in fact by receiving the Gardasil Vaccine.

This statement is reinforced by a supportive Expert Report written by Sin Hang Lee, MD, stating:

Gardasil® did cause or contributed to a myocardial infarction in the decedent, and that the second dose of Gardasil®finally caused a fatal hypotension in this case on the day of vaccination. There was no other plausible cause for the death of Joel Gomez at the night of August 19, 2013.

The record shows that Joel Gomez, the decedent, a 14-year old healthy boy who had regular visits to the pediatrician’s office for periodic check-ups since birth showed no evidence of any pre-existing health issues, specifically no evidence of cardiac abnormalities, psychological disorders or substance abuse. The teenager had been training for the high school football team from four to five hours a day for the two months prior to his death without incident.

On June 19, 2013, the boy was given the first dose of Gardasil® in his left arm in the doctor’s office. No adverse reactions were reported following this first vaccination by the boy to either his family or his physician. On August 19, 2013 the boy was given a second injection of Gardasil® as scheduled in the doctor’s office. Then he went home and went to sleep. The boy was found to be unresponsive in bed the following morning on August 20, 2013 at 7:00 a.m. by his family.

Paramedics were called in and the boy was transported to the hospital where he was pronounced dead at 9:07 a.m. on August 20, 2013.

An autopsy was performed on August 23, 2013 by a medical examiner (ME) of Los Angeles, California.

The autopsy report stated significant abnormal findings to include:

…a long narrow band of dark reddish discoloration which is somewhat darker than the rest of the myocardium, extends over a length of 6 cm and has a width of 0.4 cm extending from the anterior base of the heart almost to the apex. ..this lesion is limited to the anterior free wall. Both lungs are extremely heavy. The lung parenchyma is dark-purple-red and completely soaked with edema fluid and blood. Microscopically, a localized lesion was found in the left ventricle of the heart.

In the medical examiner’s opinion:

The Decedent died of myocarditis, which apparently was completely asymptomatic. By histology, the disease had been present for at least several days or weeks. The cause is unknown.

Dr. Lee reviewed the microscopic slides and concluded that the lesion of the heart was a healing myocardial infarct of a few weeks old after the first Gardasil® vaccination. In his opinion,

The HPV L1 gene DNA fragments bound to the aluminum adjuvant in Gardasil® can cause sudden and unexpected surge of tumor necrosis factor-α and other cytokines. Some of these cytokines released from macrophages are potent myocardial depressants, capable of causing hypotension with low cardiac perfusions in certain genetically or physically predisposed individuals.

Why is this case significant?

Myocardial Infarction

This was an obviously healthy, athletic young boy under the care of a pediatrician since birth. The myocardial infarction occurred between two injections of Gardasil as described in the medical examiner’s report. According to Dr. Lee, a healing infarct at the age of 14 is practically unheard of. In fact, Dr. Lee pointed out that the heart in this case presents a textbook description of myocardial infarction commonly observed in much older patients with a history of heart attack(s). The only factor in this boy’s life that changed was his Gardasil vaccinations.

According to the petition filed:

Petitioners contend that Joel suffered from Myocarditis which was caused in fact by the Gardasil vaccine. Petitioners contend that the logical sequence of cause and effect show that the vaccination was the reason for the death. Further supportive of the causal relationship is established by looking to the proximate temporal relationship between the vaccination and the death. The fact that Joel was a healthy 14 year old boy with no health problems is strong circumstantial evidence that the death was caused in fact by the Gardasil vaccine.

This means there is no way of knowing how many Gardasil-vaccinated girls (or boys) have developed permanent myocardial damage, whether one calls it myocarditis or infarct, either is a silent heart pathology. Is silent heart pathology no harm if the patient did not die?

In a telephone interview with Dr. Lee about the significance of this case for parents and medical professionals, Dr. Lee said:

Teenagers vaccinated with Gardasil® should stay away from competitive sports such as football for at least two months, and should have an electrocardiogram to rule out silent myocardial infarction if there is any incidence of syncope, chest discomfort, tachycardia or hypotension within two months after Gardasil® vaccination.

References:

  1. petition available on request – please email admin@sanevax.org or sanevax@gmail.com

This article in its entirety, is compliments of www.SaneVax.org

 

 

HPV Vaccines: SaneVax Message to Colombia#Family#Columbia#HPV

By Norma Erickson

 

SaneVax-FeaturedAttorney Monica Leon Del Rio is currently representing several Colombian girls who are experiencing new medical conditions after the administration of Gardasil. She recently invited me to speak to a group of esteemed public health officials, government representatives and medical people in Colombia to explain why the SaneVax team does not support HPV vaccination programs.Just prior to the time I was to address the meeting, the international conference call was disconnected. Despite multiple attempts to re-establish the connection I was not able to speak as scheduled.

Therefore, my intended message to Colombia is as follows:

SaneVax is an international non-profit organization working with representatives in over 25 countries, all of whom are concerned about HPV vaccines. The SaneVax team believes vaccines should meet four common sense criteria prior to their inclusion in mass vaccination programs. We believe they should be scientifically proven safe, affordable, necessary and effective prior to government approval.

The SaneVax Team cannot support HPV vaccination programs for many reasons.

#1 HPV VACCINES ARE NOT PROVEN SAFE

  • There are over 80 vaccines approved for use in the United States. HPV vaccines account for nearly 25% of the entire Vaccine Adverse Event Reporting System (VAERS) database. This is particularly disturbing because the VAERS system was established in 1990 and HPV vaccines were not introduced until mid-2006.
  • VAERS reports of ADEM have increased over 1,000% since the introduction of HPV vaccines; infertility reports increased 790%, reports of blindness increased 188%, and spontaneous abortions by 270%.
  • According to documents submitted to the Supreme Court in India, when 24,000 girls were injected with HPV vaccines during ‘demonstration projects’ an estimated 5% (1200) were left with chronic health problems and/or autoimmune disorders.
  • Japan withdrew the government recommendation for the administration of HPV vaccines after only 6 weeks when reports of adverse events after Gardasil were 26 times higher than the annual flu shot; reports after Cervarix were 52 times higher than the annual flu shot. 24.9% of the adverse events reported were considered serious.
  • Denmark reports that 24% of the adverse events reported after HPV vaccinations were considered serious.
  • Italy reports adverse events after HPV vaccines at a rate of 219/100,000 – ten times higher than most other vaccines administered in Italy. The cervical cancer rate in Italy is 7.7/100,000.

#2 HPV VACCINES ARE NOT AFFORDABLE

  • HPV vaccination programs do not eliminate the need for pap screening, they simply add the price of 3 injections to already overburdened healthcare systems around the globe.
  • There is an already proven safe and effective method of controlling cervical cancer in most developed countries – pap screening and good gynecological follow-up. Countries without this practice in place would be money ahead to spend their healthcare budget developing the infrastructure to provide this type of care.
  • Cervical cancer causes 2.3 deaths/100,000 women in the United States. The cost of 3 doses of HPV vaccine for 100,000 women is an estimated $30,000,000 ($100/dose) to try and eliminate less than 3 deaths which could have been avoided with pap screening and good gynecological follow-up. How many medical professionals could be trained and/or medical facilities built with that same 30 million dollars?

#3 HPV VACCINES ARE NOT NECESSARY

  • The human papillomavirus has never been proven to cause cancer by itself. Other risk factors must also be present in order to prompt the development of cancer.
  • According to the World Health Organization, only 0.15% of all people exposed to any high-risk strain of HPV will ever develop cervical cancer. The vast majority of HPV ‘infections’ are benign and cause no medical problem whatsoever.
  • HPV type prevalence varies greatly from one region to the next. Are the HPV types targeted by current vaccines the same ones prevalent in your country?
  • There is no excuse for exposing the female population of the world to the risks involved with HPV vaccination when there is an already proven safe, affordable, necessary and effective means of controlling cervical cancer.

#4 HPV VACCINES ARE NOT PROVEN EFFECTIVE

  • According to the World Health Organization, only 1% of CIN1 progresses to the next stage, only 1.5% of CIN2 progresses. Only 12% of CIN3 lesions, which are actually considered a pre-cursor to cancer. Nevertheless, the FDA allowed the manufacturers of HPV vaccines to use these often self-reversing abnormal lesions as endpoints to judge the efficacy of their products.
  • The other endpoint used to predict efficacy was antibody titers. No one has determined what level of antibodies is necessary to prevent HPV infections. It is simply assumed that the higher the antibody titer level, the better the potential protection.
  • HPV vaccines have not been clinically proven to prevent a single case of cancer.
  • There is no guarantee that eliminating one risk factor for the development of cervical cancer will have any impact on the disease incidence or mortality rate.
  • It will take more than 20 years to determine whether or not HPV vaccines perform as advertised.
  • There is no guarantee that any suppressed oncogenic HPV type will not mutate over the next 20 years and become more dangerous.

I would respectfully submit that all of these facts should be taken into consideration when evaluating the HPV vaccination program in Colombia.

Please consider every new medical condition following HPV vaccine administration to be a potential adverse event. Thorough investigations are the only way to determine the safety profile of HPV vaccines in your country.

Please take action to protect your future generation.

Halt the current HPV vaccination program until you have determined whether or not HPV vaccines are a good addition to your cervical cancer prevention program.

You must answer the question – Are HPV vaccines Safe, Affordable, Necessary and Effective in Colombia?

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

LSaneVax-Featureda abogada Mónica León Del Rio actualmente representa a varias niñas colombianas que están experimentando nuevas afecciones médicas después de la administración de Gardasil. Ella hace poco me invitó a hablar a un grupo de funcionarios de salud pública, representantes gubernamentales y personal médico en Colombia para explicar por qué el equipo SaneVax no respalda los programas de vacunación contra el VPH.Justo antes de mi participación en la conferencia internacional, se desconectó la llamada. A pesar de múltiples intentos para restablecer la conexión no pude hacer mi presentación.

Por lo tanto, mi mensaje destinado a Colombia es el siguiente:

SaneVax es una organización internacional sin ánimo de lucro que trabaja con representantes en más de 25 países, todos los cuales están preocupados acerca de las vacunas contra el VPH. El equipo SaneVax cree que las vacunas deben cumplir con 4 criterios de sentido común antes de incluirse en los programas de vacunación masiva. Creemos que deben ser demostrados científicamente que son seguras, asequibles, necesarias y eficaces antes de ser aprobadas por el gobierno.

El Equipo SaneVax no puede apoyar los programas de vacunación contra el VPH por muchas razones.

#1 No se ha demostrado que las vacunas contra el VPH sean SEGURAS

  • Hay más de 80 vacunas aprobadas para su uso en los Estados Unidos. Las vacunas contra el VPH representan casi el 25% de toda la base de datos de Eventos Adversos de Vacunas (VAERS). Esto es especialmente preocupante porque el sistema VAERS se estableció en 1990 y vacunas contra el VPH no se introdujeron hasta mediados de 2006.
  • VAERS informa que los casos de Encefalitis Aguda Diseminada se han incrementado en un 1.000% desde la introducción de vacunas contra el VPH; los informes de infertilidad se incrementaron 790%, los casos de ceguera aumentaron 188%, y los abortos espontáneos por 270%.
  • De acuerdo con los documentos presentados a la Corte Suprema de la India, cuando 24.000 niñas fueron inyectadas con vacunas contra el VPH durante los “proyectos de demostración”, se estima que un 5% (1.200) quedaron con problemas de salud crónicos y / o trastornos autoinmunes.
  • Japón retiró la recomendación del gobierno para la administración de las vacunas contra el VPH después de sólo 6 semanas, cuando los informes de eventos adversos después de la aplicación del Gardasil eran 26 veces más altos que los de la vacuna anual contra la gripe; los informes de eventos adversos después de la aplicación de Cervarix fueron 52 veces más altos que los de la vacuna anual contra la gripe. El 24,9% de los eventos adversos informados fueron considerados graves.
  • Dinamarca informa que se consideran graves un 24% de los eventos adversos informados después de la vacunación contra el VPH.
  • Italia informa de los eventos adversos después de la aplicación de las vacunas contra el VPH a una tasa del 219/100 000 – diez veces más alta que la mayoría de las vacunas administradas en Italia. La tasa de cáncer de cuello uterino en Italia es de 7,7 / 100.000.

#2 Las vacunas contra el VPH NO SON ADSEQUIBLES

  • Los programas de vacunación contra el VPH no eliminan la necesidad de las pruebas de detección de Papanicolaou (citología vaginal), inclusive hay que añadir el precio de 3 inyecciones que se sobrecargan a los sistemas sanitarios de todo el mundo.
  • La detección mediante la prueba de citología vagina (prueba de Papanicolaou) es un método seguro y eficaz ya probado para controlar el cáncer cervical en los países más desarrollados incluyendo el buen seguimiento ginecológico.
  • El cáncer cervical provoca 2,3 muertes / 100.000 mujeres en los Estados Unidos. El costo de 3 dosis de la vacuna contra el VPH para 100.000 mujeres tiene un costo estimado de $ 30.000.000 ($ 100 / dosis) para tratar de eliminar menos de 3 muertes que podrían haberse evitado con la prueba de Papanicolaou y un buen seguimiento ginecológico. ¿Cuántos profesionales de la medicina podrían ser capacitados o cuántas instalaciones médicas se podrían construir con los mismos 30 millones de dólares?

#3 Las vacunas contra el VPH no son necesarias

  • El virus del papiloma humano nunca se ha demostrado que cause el cáncer por sí mismo. Otros factores de riesgo también deben estar presentes para facilitar el desarrollo del cáncer.
  • De acuerdo con la Organización Mundial de la Salud, sólo el 0,15% de todas las personas expuestas a cualquier cepa de alto riesgo de VPH desarrollarán cáncer cervical. La gran mayoría de los ”infecciones” por VPH son benignas y no causan ningún problema médico.
  • La prevalencia del tipo de VPH varía mucho de una región a otra. ¿Son los tipos de VPH que son el blanco de las vacunas actuales los mismos que prevalecen en su país?
  • No hay excusa para la exposición de la población femenina del mundo a los riesgos que implica la vacunación contra el VPH cuando ya hay métodos seguros, asequibles, necesarios y efectivos probados para el control del cáncer cervical.

#4 Las vacunas contra el VPH no tienen una eficacia demostrada

  • De acuerdo con la Organización Mundial de la Salud, sólo el 1% de Neoplasia Intraepitelial Cervical 1 (CIN1) avanza a la siguiente etapa CIN2 y de esta sólo el 1,5% progresa. Solo un 12% de las lesiones CIN3 son en verdad consideradas como precursoras del cáncer. Sin embargo, la FDA permitió a los fabricantes de vacunas contra el VPH utilizar estas lesiones anormales que a menudo se curan por sí mismas como criterios para juzgar la eficacia de la vacuna.
  • El otro criterio de valoración utilizado para predecir la eficacia fueron las medidas de anticuerpos. Nadie ha determinado cuál es el nivel de anticuerpos necesario para prevenir las infecciones por VPH. Simplemente se supone que el nivel más alto de anticuerpos es potencialmente mejor.
  • No se ha demostrado clínicamente que ninguna vacuna contra el VPH prevenga un solo caso de cáncer.
  • No hay garantía de que la eliminación de un factor de riesgo para el desarrollo de cáncer de cuello uterino (infección por VPH) tendrá impactos sobre la incidencia de la enfermedad o tasa de mortalidad.
  • Tardará más de 20 años para determinarse si las vacunas contra el VPH funcionan o no como se anuncia.
  • No hay garantía de que cualquier tipo de VPH oncogénico suprimido por la vacuna no va a mutar en los próximos 20 años y ser más peligroso.

Me permito pedir respetuosamente que todos estos hechos sean tenidos en cuenta al evaluar el programa de vacunación contra el VPH en Colombia.

Por favor consideren que cada nuevo caso de anormalidad médica luego de la administración de la vacuna contra el VPH puede ser un evento adverso a la misma. Las investigaciones exhaustivas son la única manera de determinar el perfil de seguridad de las vacunas contra el VPH en su país.

Por favor, tomen medidas para proteger sus generaciones futuras.

Detengan el programa de vacunación contra el VPH actual hasta que se haya determinado si las vacunas contra el VPH son una buena adición al programa de prevención de cáncer de cuello uterino.

Deben responder a la pregunta – ¿Son las vacunas contra el VPH seguras, asequibles, necesarias y eficaces en Colombia?

 

 

 

This article in it’s entirety, is compliments of www.SaneVax.org

HPV Vaccination Program in Colombia: Undermining the Truth?#Family#Vaccines#Columbia

By Norma Erickson

SaneVax-FeaturedHundreds of young women in Carmen de Bolivar, Colombia ended up in hospitals since the administration of the second dose of Gardasil beginning in schools on March 20, 2014. Local newspapers report as many as 700 girls being sent to emergency rooms after receiving Gardasil over the last few months.

According to a local school teacher:

The girls in Carmen de Bolivar received their first dose of Gardasil in July 2013, after which reported reactions were similar to other vaccines (redness, swelling, pain at the injection site, etc…). The second dose was administered on the 20th of March 2014. Several girls reacted immediately and much more severely, reporting dizziness, syncope, and severe headaches. By May 29th to the 30th, the situation had turned into a full-blown crisis with scores of girls being admitted to local emergency room facilities to be treated for fainting, shortness of breath, weakness in the limbs etc…

No one seems to know what instigated this epidemic number of hospital visits. Government health officials emphatically denied that Gardasil could be causing the extraordinary number of new medical conditions. Instead, they put forth theories such as lead poisoning, mass hysteria and even too much Ouija board use.

Parents of the affected girls did not agree with any of these theories. They knew the only thing that had recently changed in their daughters’ life was the administration of the second dose of the HPV vaccine, Gardasil.

Hundreds of parents took to the streets in peaceful demonstrations to demand investigations; others burned tires in protest, blocking a main road connecting a coastal town with the interior. For the first time in the history of Colombia, perhaps the world, parents launched massive public protests over the administration of a vaccine that is apparently making people sick instead of protecting them. (read more)

Parents of affected children suspected Health Minister Alejandro Gaviria of being less than truthful, being misinformed, or simply protecting special interest groups supporting the use of Gardasil and they were not shy about stating their suspicions in any public forum they could gain access to.

Health Minister Gaviria accused media representatives of contributing to the creation of an epidemic of ’mass hysteria’ and publicly requested journalists and media personnel to exercise ’more responsible journalism.’

Dr. Nubia Muñoz Calero

Enter Nobel-prize nominee, Dr. Nubia Muñoz Calero

Sunday, October 5, 2014, Alda Mera, reporter for El Pais, published an article titled, The HPV vaccine saves lives, Nubia Muñoz Calero. Reporter Alda Mera apparently thought there was no one better to allay the fears of Colombian parents than an epidemiologist who had been born, raised and educated in Colombia, who had participated in cancer research for more than 30 years and been nominated to receive a Nobel Prize for her work. This medical scientist was Dr. Nubia Muñoz Calero. (read her biography here)

Unfortunately, the article published as a result of reporter Alda Mera’s interview with Dr. Nubia Muñoz Calero continues to market HPV vaccines via fear, not facts.

Please examine the statements from Alda’s article below when compared with documented factual information:

According to Dr. Muñoz Calero, when asked if Colombia understands the importance of her discovery that HPV causes cervical cancer, the good doctor states, ”I am not the inventor of (HPV) vaccines, pharmaceutical companies developed them. I have no commercial interest in them.”

FACT:  What Dr. Muñoz Calero fails to mention is that she is a member of the Merck HPV Global Advisory Board. This may not be what one would technically call a commercial interest. However, it does constitute a substantial conflict of interest when one is being portrayed as an independent scientific expert. (verify here) Why did Reporter Alda Mera not disclose this information?

According to Dr. Muñoz Calero, her contribution was to demonstrate with well-planned epidemiological studies that the human papillomavirus is the main and necessary cause of cervical cancer.

FACT:  Epidemiological studies never prove causation. They cannot prove that a specific risk factor actually causes the disease being studied. Epidemiological evidence can only show that this risk factor is associated (correlated) with a higher incidence of disease in the population exposed to that risk factor. The higher the correlation the more certain the association, but an epidemiological study cannot prove causation. (verify here)

It is also important to note that papers published prior to FDA approval of Gardasil refer to HPV as being ’associated with’ the development of cervical cancer. It was only after FDA approval of Gardasil that ’scientific’ papers began to refer to human papillomavirus as being ’causally associated’ with the development of cervical cancer. This phrase soon morphed into HPV being ’the main and necessary cause’ of cervical cancer. (verify here, in Dr. Muñoz Calero’s own published paper – simply scroll through the referenced papers and look at their dates of publication.)

According to Dr. Muñoz Calero, she had helped identify the two types of HPV (human papillomavirus) responsible for 70% of cervical cancer.

FACT:  What the esteemed doctor failed to mention is the fact that the two types identified may not be the prevalent types in the Colombian population. If HPV 16/18 are not the prevalent types in Colombian women, any effect Gardasil may have on the prevalence of cervical cancer in her country would diminish substantially. (verify here)

According to Dr. Muñoz Calero, when asked about the safety demonstrated during the clinical trials of Gardasil, she stated, ”As an intramuscular injection (Gardasil) produces some pain in 80% of girls, heat and redness in the arm. A small percentage have headaches and fevers, 10% for maybe one or two days. But these 40,000 women (who participated in clinical trials) did not suffer syncope, fainting, or diseases that (are) now blamed on the vaccine.

FACT:  According to documentation presented to the FDA prior to Gardasil approval in the United States, 73.3% of clinical trial participants who received Gardasil reported new medical conditions after vaccine administration. It is interesting to note that 76.3% of those who received the so-called ’placebo’ also reported new medical conditions after injection. The problem here is that the ’placebo’ used was not an inert substance – it consisted of the brand new (not safety tested) proprietary aluminum adjuvant Merck developed for use in Gardasil and a ’carrier’ solution with undisclosed ingredients. The only thing these clinical trials proved was that Gardasil was no less dangerous than the adjuvant used in Gardasil. Many of the new medical conditions reported during clinical trials are the same ones being reported around the world after Gardasil administration. (verify here) (list of reported new medical conditions from clinical trials here)

According to Dr. Muñoz Calero, when asked whether Gardasil had been rushed to market, stated that the laboratories created the first human papillomavirus vaccine at the end of the 90’s, and began phase I and II clinical trials before 2000.

FACT: Merck’s development program for the HPV quadrivalent vaccine for prevention of cervical cancer was granted fast track designation in 2002. Merck initiated phase 3 clinical trials of the HPV quadrivalent vaccine in 2002. (verify here) This fast track designation was granted despite the fact that Merck’s proposed vaccine did not meet any of the criteria required for fast track approval. (verify here)

According to Dr. Muñoz Calero, when asked about the adverse reactions being reported in Colombia, says she does not know in detail what is happening in Carmen de Bolivar because she does not live in the country; but based on what she’s read and been told by colleagues….200,000 million doses have been distributed (not necessarily administered) in the world. WHO, PAHO, FDA and EMA say that Gardasil is safe and there is no scientific evidence showing (that it) triggers autoimmune diseases (Guillán-Barre syndrome, multiple sclerosis, transverse myelitis).

FACT:  There may be no concrete scientific proof that HPV vaccines are triggering and/or causing the adverse events being reported in every country where they are administered. However, there is also no scientific proof that HPV vaccines are NOT causing these new medical conditions either. There is no such thing as an epidemic of coincidence.

The SaneVax team would like Dr. Muñoz Calero to explain why biologically plausible mechanisms of action that could explain new medical conditions occurring after the administration of HPV vaccines presented by scientists and medical researchers around the globe is not being investigated thoroughly by any of the alphabet organizations she mentions which all have vested interests in mass administration of one of the most expensive vaccines ever produced. (verify here and here)

Near the end of the interview, Dr. Muñoz Calero is asked if it would be a good idea to stop mass HPV vaccinations in Colombia until after investigations to determine which children are at risk for adverse reactions. She states:

No. It would be a mistake to stop the program. Countries that achieve the highest coverage are those with school-based programs. What I recommend is to increase education programs for physicians, media, and communities. Make them understand that this vaccine is the best weapon against cervical cancer.

Dr. Muñoz Calero, since when is it a mistake to apply the precautionary principle to the administration of a medical intervention of any kind?

Anyone with an ounce of compassion would be fighting to protect the continued health and well-being of the young girls in their native land; NOT fighting to preserve the uptake of a vaccine which might be responsible for epidemic numbers of health problems.

The new medical conditions occurring after Gardasil administration must be investigated thoroughly before any more young women are subjected to devastating potential risks in exchange for the highly debatable promise of a reward 20 years down the road.

The latest ’medical miracle’ can wait until after independent investigations determine it to be safe.

By the way, there is a huge difference between being ’anti-vaccine’ and supporting vaccine safety.

If a pharmaceutical company cannot market their products based on facts, they should not be allowed to market them at all!

This article in it’s entirety, is compliments of www.SaneVax.org